Post on 08-Jun-2020
General Overview of ImmunologyGeneral Overview of Immunology
Kimberly S. Schluns, Ph.D.Associate ProfessorDepartment of ImmunologyUT MD Anderson Cancer Center
Objectives
• Describe differences between innate and adaptive immune responses
• Describe the immune cells that mediate and regulate immune responses
• Define common terminology
• Explain how immune cells recognize and respond to foreign entities
• Relate basic concepts of immunology to its applications in immunotherapy
Immune System- Body’s defense against infection
Late 1700s Edward Jenner observed that prior history of a mild disease of cowpox (vaccinia) conferred protection against fatal smallpox
Vaccination inoculation of healthy people with weak or attenuated agents that cause disease.
Disease causing agents were unknown.
Pathogens:Viruses, bacteria, fungi, parasites
What was the mechanism of protection?
Definition: Immunity- the state of being immune from, insusceptible to, or protected from a particular disease or the like.
Immune Reponses
AdaptiveInnate
•Always available
•First line of defense
•Specific for general types of pathogens but not an individual pathogen
•Does not lead to lasting immunity
•Develops during lifetime as an adaptation to infections with pathogens
•Is antigen specific (ex. H1N1 strain of flu but not all Influenza strains)
•Confers long lasting immunity
Function of Immune Reponses
•Immune Recognition-detects the presence of infection.
•Immune Effector Function- contains and eliminate infection (degradative enzymes, complement, Ab, cell lysis)
•Immune Regulation-controls immune response to prevent damage
•Immunological Memory- protects against recurring disease to the same pathogen
All are accomplished by innate and adaptive immune cells except immunological memory
Immune cells are derived
from stem cells in the bone marrow
All are considered -hematopoietic cells -leukocytes (very general term)
The myeloid lineage comprises most of the cells of the innate immune system
Granulocytes
Neutrophils, Eosinophils, Basophils are sometimes referred to aspolymorphonuclear leukocytes:
Short lived cells that possess granules containing degradative enzymes and anti-microbial substances
Allergy (Blood mast cells)
Neutrophils, Macrophages, and Dendritic Cells
Reside in tissues
*
*
(small particles)
Main role is not clearance of pathogen but rather lymphocyte activation
Dendritic cells and macrophages are two types of professional antigen presenting cells (APCs)
Phagocytes
Three Main Antigen Presenting Cells (APCs)
Immature DCs very efficient at Ag processing (in tissues)
Mature DCs very efficient at Ag presentation (in LNs)
Professional APCs present Ag to naïve T cells and induce activation
LymphocytesGenerally: small inactive cells
3 Types:T and B cells-mediate adaptive responses(recognize veryspecific antigens via antigen-receptors)
NK cells-mediate innate responses(recognize general features on tumor and virus-infected cells)
Adaptive Innate
How do these two arms recognize foreign Ag/Cells?
Adaptive and innate immune cells in the hematopoietic lineage
PAMP Receptors are enriched on, but are not restricted to innateimmune cells
Innate responses are initiated upon recognition of common features of pathogens (PAMPs)
by pattern recognition receptors
PAMPs (Pathogen-associated molecule patterns)
-examples: lipopolysaccride on bacterial cell walls (LPS), unmethylated CpG DNA, mannose-rich oligosaccarides
Infectious agents first activate innate immune cells resulting in an inflammatory response
Chemokines- group of cytokines that attract other immune cells
Cytokines-proteins that immune cells use to communicate/regulate other immune cells, not all cytokines are inflammatory
adaptivecells
arrivelater
PAMPs are responsible for effectiveness of adjuvants
Purified proteins
killed bacteria or bacterial extracts
+purified protein
Obtain response to purified protein
Bacterial proteins stimulate DCs making them efficient APCs for lymphocytes
poorly immunogenic
DCs are important for initiating adaptive immune responses
This is an important bridge between innate and adap tive responses;a failure to stimulate innate immune cells can lead to poor T cell and
B cell responses.
Natural Killer Cells (NK cells)
NK cells express inhibitory and activating receptors that recognize self MHC class I and NK cell receptor ligands respectively
No NK cell activation
Preformed granules
Natural Killer Cells (NK cells)
Tumor cells, virus-infected cells, and transplanted cells are targets of NK cell killing because of decreased MHC Class I
NK cell activation
/DC
CD8
Memory CD8 T cell
Memory CD4 T cellMemory
Adaptive Immune Responses
Antibodies present in blood allow immunity to be transferred via proteins
Immunity is mediated by cells
Antigen Receptors
Antibody (Ab)
(Cell surface only)(Cell surface and secreted)
T cell Receptor (TCR)
Antigen Recognition by Antibodies
(Ag)
(Ab)
Ab recognize portions of proteins in native structures, not processed proteins (may not be continuous portion of protein)
T cell Receptor (TCR) recognize processed proteins
Understand what “epitope” means-how are TCR epitopes different from Ab epitopes?
(MHC= Major Histocompatibility Complex)
MHC Class I-expressed by all nucleated cells-presents peptides derived from endogenous proteins-MHC Class I proteins are also recognized by NK cell s
MHC Class I presents peptide antigens to CD8 T cells
MHC Class II presents peptide antigens to CD4 T cells
MHC Class II -typically expressed by professional AP Cs-presents peptides derived from exogenous proteins
Macrophages:
B cells:
Each lymphocyte has a unique specificity
-Generation of vast pool of cells
Immature cells(non-functional)
Development
-Shaping the repertoire
Circulating mature naïve cells
One barrier to inducing responses against tumor cells
Hogquist, K.A. et al 2005
Only a small portion of thymocytes become mature T cells
TCR Affinity
Number of Thymocytes
DeathBy clonal deletion
Death by neglect
Positive Selection
Naïve T cells
Hogquist, K.A. et al 2005
Some T cells escape negative selection
TCR Affinity
Number of Thymocytes
DeathBy clonal deletion
Death by neglect
Positive Selection
T cells(tolerant orregulatory)
Escape
Naïve T cells
Clonal Expansion
Cells that recognize a specific Ag are very rare
These all have the same specificity
What is the purpose of clonal expansion?
Each T/B cell has unique Ag R
T/B cells that recognize self are eliminated
Recognition of Ag lead to activation
Effectors derived from parent cell all have the same Ag R
Central Principle of Adaptive Immunity
Primary Lymphoid Tissues
SecondaryLymphoid Tissues
Where does lymphocyte development and activation occur?
T cells develop in the Thymus
B cells develop in the bone marrow
T and B cell stimulation occur in the lymph nodes and spleen
Spleen
BM
Thymus
Primary and Secondary Lymphoid Organs
LN
Lymph Nodes collect lymph and antigen
from peripheral sites
The Spleen collects antigens from circulating
blood
LNs are prime site for lymphocyte stimulation
Stimulation of Lymphocytes
Both T and B cells require stimulation thru AgR (Signal 1) and additional costimulation (Signal 2) Absence of costimulation leads to tolerance
*Must be mature DC
T cell Activation
Results in:1.Expansion2.Acquisition of
effector functions
“Naive”
“Activated” or“Effectors”
Effector Mechanisms of Adaptive Immunity
CD8+ T Cells (Cytotoxic T cells)
• Recognize transformed and virus infected cells
• Confer cytolytic activity
–Release perforin, granzyme,
IFN-γ, γ, γ, γ, TNF-αααα– Induce apoptosis
• Majority of cancer vaccines are designed to stimulate CD8T cell response
Effector Mechanisms of Adaptive Immunity
CD4+ Helper T CellsTh1
Th2
• Regulate development and
persistence of cell-
mediated immunity
• IL-2, INF-γ
• Enhance humoral immune
responses; B cell
maturation, clonal
expansion, class switching
• IL-4, IL-5, IL-6, IL-10, IL-13
Effector Mechanisms of Adaptive Immunity
CD4+ Helper T Cells
Th17 Treg
• Play role in inflammation and
tissue injury
• Stimulates anti-microbial
responses by epithelial cells
• Recruits, stimulate
Neutrophils
• May mediate regression of
tumors
• IL-17, IL-22
• Recognize self Ag
• inhibit or suppress other
adaptive immune responses
• IL-10, TGF-β
Effector Mechanisms of Adaptive Immunity
Ab help eliminate extracellular pathogens
B Cells
Ab can be used to eliminate large subsets of cells-Example:Rituximab= Ab against B cell cell surface molecule
Lymphocyte Activation
Results in:1.Expansion2.Acquisition of effector functions
3. ?
“Naive”
“Activated” or“Effectors”
What happens to T cells and B cells after antigen is gone?
Activation of B cells generates Ab -producing plasma cells and memory B cells
(Lymphoblast Plasmablast)
Earlier phases are dominated by IgM, later IgG and IgA are predominant
Cytokines also induce class switching
Time
pathogen
Num
ber
of A
g-sp
ecifi
c T
cel
lsNaïve Effector Memory
30 days(Level of detection)
Note: level
expansion contraction
Generation of memory lymphocytes
Time Ag
Num
ber
of A
g-sp
ecifi
c ly
mph
ocyt
es
Ag (Challenge)
secondary responseprimary response
Why is a secondary immune response larger, faster, and more effective?
Significance of Immunological Memory
Larger, faster, more effective
Efficacy of memory T cells
• Ag-specific memory T cells are present at higher levels than naive T cells
• Reactivation of memory T cells occurs within a few hours, while naïve T cell activation require days
• Memory T cells are anatomically dispersed
• Memory T cells are long-lived, self renewing, and Ag-independent
Some activated T cells become effectors while others become memory T cells
Memory T cells are heterogeneous in their migratory and functional abilities
Effector memory T cells •L-selectin- CCR7-•Preferentially migrate through tissues•Possess immediate effector functions
Central memory T cells •L-selectin+ CCR7+•Preferentially migrate to secondary lymph. organs•Respond optimally to challenge
With the increased effector functions and non-lymphoid localization, effector memory T cells (Tem) are thought to act as a first line of defense; whereas central memory T cells (Tcm) may provide more long lasting protection.
MemoryPrecursorsEffectors
Short livedEffectors
Effector and central memory T cells are both derived from memory precursor
CD62L- Memory
CD62L+ Memory
IL-7Rααααhi
IL-7Rααααlo
Too much Ag stimulation can lead to the generation of dysfunctional T cells or the absence of memory T cells
Observed in tumors and chronic infections
Exhausted T cells often show a specific phenotypic signature (PD-1, Tim 3, LAG-3)
TimeAg stimulation
Num
ber
of A
g-sp
ecifi
c C
D8
T c
ells
Dynamics of a T Cell Response
Naïve Effector Memory
functional
suboptimal
30 days(Level of detection)
chronic
Immune responses can be beneficial or harmful
Immune Regulation
T regulatory cells•Inhibit or suppress other adaptive immune responses•Multiple subsets, with different developmental origins•CD4+Foxp3+ T regs, recognize self Ag, produce TGF-ββββ and IL-10, are generated during development or induced from naïve T cells in the periphery•TH3 cells- produce TGF-ββββ and IL-10,,,, found in mucosa•Enriched in the tumor microenvironment
Myeloid-derived Suppressor cells•Heterogeneous, immature myeloid phenotype•Includes tumor-associated macrophages, which produce IL-10 and TGF-β,β,β,β, but not cytolytic factors•Suppress via arginase, iNOS•Expand during inflammation, infection, and cancer•Enriched in the tumor microenvironment
Function of Immune Reponses
•Immune RecognitionVarious immune cells use different mechanisms to recognize foreign entities- TLR, NK cell R, Ab, TCR
•Immune Effector FunctionPhagocytosis, Ab neutralization, cytolysis, cytokines
•Immunological Memory T cells and B cells provide long term protection against recurrences
•Immune RegulationTregs, myeloid-derived suppressor cells
Questions
1. Innate immune responses
a)are initiated after adaptive immune
responses are elicited
b)become more efficient throughout one’s
lifetime
c)are important for successful vaccination
d)are capable of distinguishing mutated
proteins expressed by tumors
e)none of the above
Questions
2. Adaptive immune responsesa)are present at birthb)are specific for general types of pathogensc)are capable of generating long lasting immunityd)are mediated by NK cells and T cellse)none of the above
Questions
3. T cellsa)each express antigen receptors with one unique specificityb)that are specific for self-proteins are preserved during developmentc)that are naive undergo activation within a few hoursd)require stimulation through only their TCR receptor for efficient activatione)none of the above
Questions
4. Regarding Antigen Recognition: a)T cell antigen receptors (TCR) recognize proteins in their natural structureb)Antibodies recognize processed peptide antigens presented on the cell surfacec)TCRs recognize peptide antigens presented by MHC Class I and II moleculesd)Antibodies are expressed only as a soluble forme)none of the above